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Dengue vaccine–induced CD8+ T cell immunity confers protection in the context of enhancing, interfering maternal antibodies
Jian Hang Lam, … , Eng Eong Ooi, Sylvie Alonso
Jian Hang Lam, … , Eng Eong Ooi, Sylvie Alonso
Published December 21, 2017
Citation Information: JCI Insight. 2017;2(24):e94500. https://doi.org/10.1172/jci.insight.94500.
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Research Article Infectious disease Vaccines

Dengue vaccine–induced CD8+ T cell immunity confers protection in the context of enhancing, interfering maternal antibodies

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Abstract

Declining levels of maternal antibodies were shown to sensitize infants born to dengue-immune mothers to severe disease during primary infection, through the process of antibody-dependent enhancement of infection (ADE). With the recent approval for human use of Sanofi-Pasteur’s chimeric dengue vaccine CYD-TDV and several vaccine candidates in clinical development, the scenario of infants born to vaccinated mothers has become a reality. This raises 2 questions: will declining levels of maternal vaccine-induced antibodies cause ADE; and, will maternal antibodies interfere with vaccination efficacy in the infant? To address these questions, the above scenario was modeled in mice. Type I IFN–deficient female mice were immunized with live attenuated DENV2 PDK53, the core component of the tetravalent DENVax candidate currently under clinical development. Pups born to PDK53-immunized dams acquired maternal antibodies that strongly neutralized parental strain 16681, but not the heterologous DENV2 strain D2Y98P-PP1, and instead caused ADE during primary infection with this strain. Furthermore, pups failed to seroconvert after PDK53 vaccination, owing to maternal antibody interference. However, a cross-protective multifunctional CD8+ T cell response did develop. Thus, our work advocates for the development of dengue vaccine candidates that induce protective CD8+ T cells despite the presence of enhancing, interfering maternal antibodies.

Authors

Jian Hang Lam, Yen Leong Chua, Pei Xuan Lee, Julia María Martínez Gómez, Eng Eong Ooi, Sylvie Alonso

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Figure 3

Antibody responses of pups immunized with PDK53.

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Antibody responses of pups immunized with PDK53.
(A) PRNT50 titers again...
(A) PRNT50 titers against strain 16681. Pups (n = 6) born to naive or to PDK53-immunized dams were immunized at 3 weeks of age; prevaccination and postvaccination titers were assessed at 3 and 6 weeks, respectively. Each data point represents 1 mouse; short lines represent medians and interquartile ranges. Mann-Whitney test was performed between 3- and 6-wko sera for each group. (B) DENV2 NS1–specific (αNS1) IgG titers. (C) PRNT50 titers against strain D2Y98P-PP1. Sera were pooled at each time point. **P ≤ 0.01. Data are representative of 2 independent experiments.

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